Imago BioSciences Presents Positive Data from Ongoing Phase 2 Study of Bomedemstat in Essential Thrombocythemia at ASH 2022
December 12 2022 - 11:30AM
Imago BioSciences, Inc. (“Imago”) (Nasdaq: IMGO), a clinical-stage
biopharmaceutical company discovering and developing new medicines
for the treatment of myeloproliferative neoplasms (MPNs) and other
bone marrow diseases, today presented positive data from its
ongoing global Phase 2 clinical study evaluating bomedemstat in
patients with essential thrombocythemia (ET) who have failed at
least one standard of care.
The data were presented in an oral presentation
session during the 64th American Society of Hematology Annual
Meeting and Exposition (ASH) taking place 10-13 December 2022. A
Phase 2 data set with a cut-off date of 29 April 2022 was
previously presented at the 30th European Hematology Association
Annual Meeting and congress (EHA) in June 2022.
Updated Highlights (available data as of
18 October 2022)
-
Of the 62 Patients treated with bomedemstat for more than 24 weeks:
-
100% (62/62) achieved platelet count reduction to ≤ 400 x
109/L.
-
95% (59/62) achieved platelet count reduction to ≤ 400 x 109/L in
the absence of thromboembolic events.
-
89% (25/28) of the 28 patients treated with bomedemstat for at
least 48 weeks achieved a durable response by week 48, defined as
platelet count of ≤ 400 x 109/L for ≥ 12 weeks.
-
Of the 12 patients with baseline Total Symptom Scores (TSS) greater
than 20:
-
75% (9/12) showed a decrease in TSS.
-
67% (8/12) showed improvements ≥ 10 points.
-
Platelet response rate was 100% across all genotypes identified in
the study (JAK2V617F, CALR, MPL, triple negative and no
mutations). Further, 67% (20/30) patients demonstrated a net
decrease in mutation allele frequencies including both CALR and
JAK2.
-
100% (5/5) patients with baseline loss of heterozygosity and
follow-up samples demonstrated a reduction in homozygous mutant
granulocytes and mutant allele frequencies.
“We are delighted to share the most recent data
from our ongoing Phase 2 study of bomedemstat in patients with ET,
which has notably achieved platelet count reductions to below 400 x
109/L in every patient treated for at least 24 weeks,” said Hugh
Young Rienhoff, Jr., M.D., Chief Executive Officer of Imago
BioSciences. “We are intrigued by the observation in granulocytes
that patients homozygous for a driver mutation at baseline showed
at follow-up a significant reduction in the proportion of
homozygous cells, some reduced to the limit of detection,
regardless of the driver mutation. The impact of bomedemstat on
mutant stem cell population is currently being assayed.
Additionally, we recently conducted an End-of-Phase 2 meeting with
the FDA where we aligned on a strategy for the bomedemstat Phase 3
registrational program in ET.”
Safety and Tolerability
-
Bomedemstat was generally well-tolerated with no safety signals
identified per the Safety Advisory Board.
-
The most common adverse events (AEs)(>20%) regardless of
causality were dysgeusia, constipation, thrombocytopenia,
arthralgia, fatigue, contusion and diarrhea.
-
There were 38 reported serious adverse events (SAEs), 7 of which
were deemed drug-related by the investigator in 5% (4/73) of
patients.
-
20 patients have discontinued treatment, with 10 due to AEs, 1
death from aspiration pneumonia unrelated to bomedemstat, 7 due to
withdrawal of consent, 1 due to investigator decision, and 1 due to
disease progression.
Details on the Imago ASH Oral
Presentation
Oral Presentation
Title: “A Phase 2 Study of the LSD1 Inhibitor
Bomedemstat (IMG-7289) for the Treatment of Essential
Thrombocythemia (ET)”Session Name: Myeloproliferative
Syndromes: Clinical and Epidemiological: Novel Therapies
and Surrogate Endpoints in ET and PVPresentation
Date/Time: Monday, December 12, 2022, at 11:45 AM
ETLocation: Ernest N. Morial Convention
Center, 217-219Presenting Author: Harinder
Gill, Queen Mary Hospital University of Hong Kong
For further details, please see the ASH 2022
abstract and presentation on the Imago website here.
About Imago BioSciencesImago
BioSciences is a clinical-stage biopharmaceutical company
discovering and developing novel small molecule product candidates
that target lysine-specific demethylase 1 (LSD1), an enzyme that
plays a central role in the production of blood cells in the bone
marrow. Imago is focused on improving the quality and length of
life for patients with cancer and bone marrow diseases.
Bomedemstat, an orally available, small molecule inhibitor of LSD1,
is the lead product candidate discovered by Imago for the treatment
of certain myeloproliferative neoplasms (MPNs), a family of
related, chronic cancers of the bone marrow. Imago is evaluating
Bomedemstat as a potentially disease-modifying therapy in two Phase
2 clinical trials for the treatment of essential thrombocythemia
(NCT04254978) and myelofibrosis (NCT03136185). Bomedemstat
has U.S. FDA Orphan Drug and Fast Track Designation for
the treatment of ET and MF, European Medicines
Agency (EMA) Orphan Designation for the treatment of ET and
MF, and PRIority MEdicines (PRIME) Designation by the EMA for the
treatment of MF. Imago is based in Redwood City, California.
To learn more, visit www.imagobio.com,
www.myelofibrosisclinicalstudy.com, www.etclinicalstudy.com
and follow us on Twitter @imagobiorx, Facebook and LinkedIn.
Forward Looking Statements All
statements, other than statements of historical facts, contained in
this press release, including statements regarding the results,
conduct, progress and timing of Imago clinical trials, the
regulatory approval path for Bomedemstat, and plans for future
operations and information related to Imago, are forward-looking
statements. Any forward-looking statements are based on
management’s current expectations of future events and are subject
to a number of risks and uncertainties that could cause actual
results to differ materially and adversely from those set forth in,
or implied by, such forward-looking statements. These risks and
uncertainties include, but are not limited to, Imago’s limited
operating history and lack of products for commercial sale; Imago’s
dependence on development, regulatory approval and
commercialization of its product candidates; difficulties in
enrolling patients and risks of substantial delays in its clinical
trials; Imago’s minimal control over product candidates in
investigator-initiated clinical trials; uncertainties in the cost
and outcomes of its clinical studies and the acceptance for
presentation at medical meetings of data from such clinical
studies; uncertainties in the regulatory review and approval of
Imago’s product candidates if its pivotal studies are positive;
potentially material changes to the interim, top-line and
preliminary data from its clinical trials; potential undesirable
effects of Imago’s product candidates and safety or supply issues,
in each case with respect to its product candidates alone or in
combination with other compounds or products; Imago’s potential
inability to obtain and maintain orphan drug designation and delays
in approvals despite FDA Fast Track designation for expedited
review; risks related to clinical trials outside of the United
States; Imago’s need to manufacture adequate supplies, including
multiple batches of Bomedemstat, using a commercial current Good
Manufacturing Practice; risks related to information technology
system and cybersecurity; risks related to misconduct of Imago’s
employees and independent contractors; risks related to hazardous
materials and Imago’s compliance with environmental laws and
regulations; risks related to litigation and other claims; risks
related to reliance on third parties to conduct and support
preclinical studies and clinical trials, and to manufacture Imago’s
product candidates; risks related to third-party intellectual
property infringement claims and Imago’s ability to protect its own
intellectual property; risks related to governmental policies and
regulations, including with respect to drug prices and
reimbursement, and changes thereof.
Further descriptions of risks and uncertainties
relating to Imago can be found in Imago’s Quarterly Report on Form
10-Q for the quarter ended September 30, 2022, its Annual Report on
Form 10-K for the year ended December 31, 2021 and subsequent
Current Reports on Form 8-K, all of which are filed with the SEC
and available at www.sec.gov and
https://ir.imagobio.com/financial-information/sec-filings.
You should not place undue reliance on any
forward-looking statements. Forward looking statements should not
be read as a guarantee of future performance or results and will
not necessarily be accurate indications of the times at, or by,
which such performance or results will be achieved, if at all.
Except as required by law, Imago does not undertake any obligation
to publicly update or revise any forward-looking statement, whether
as a result of new information, future developments or
otherwise.
Contacts:
Media Contact: Will ZasadnyEvoke
Canalewill.zasadny@evokegroup.com
Investor Contact:Laurence WattsGilmartin Group,
LLC.Laurence@gilmartinir.com
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